The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the Liver

The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the Liver

PPARα and HNF4α are nuclear receptors that control gene transcription by direct binding to specific nucleotide sequences. Using transgenic mice deficient for either PPARα or HNF4α, we show that the expression of the peroxisomal 3-keto-acyl-CoA thiolase B (Thb) is under the dependence of these two t...

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Main Authors: J. Chamouton, F. Hansmannel, J. A. Bonzo, M. C. Clémencet, G. Chevillard, M. Battle, P. Martin, T. Pineau, S. Duncan, F. J. Gonzalez, N. Latruffe, S. Mandard, V. Nicolas-Francès
Format: Article
Language:English
Published: Hindawi Limited 2010-01-01
Series:PPAR Research
Online Access:http://dx.doi.org/10.1155/2010/352957
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spelling doaj-141d349833d64e9e805c52f7ebe1ae932020-11-24T23:44:08ZengHindawi LimitedPPAR Research1687-47571687-47652010-01-01201010.1155/2010/352957352957The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the LiverJ. Chamouton0F. Hansmannel1J. A. Bonzo2M. C. Clémencet3G. Chevillard4M. Battle5P. Martin6T. Pineau7S. Duncan8F. J. Gonzalez9N. Latruffe10S. Mandard11V. Nicolas-Francès12Centre de Recherche, INSERM U866, LBMN 6, Boulevard Gabriel, 21000 Dijon, FranceCentre de Recherche, INSERM U866, LBMN 6, Boulevard Gabriel, 21000 Dijon, FranceLaboratory of Metabolism, Division of Basic Sciences, National Cancer Institute, Bethesda, MD 20892, USACentre de Recherche, INSERM U866, LBMN 6, Boulevard Gabriel, 21000 Dijon, FranceCentre de Recherche, INSERM U866, LBMN 6, Boulevard Gabriel, 21000 Dijon, FranceDepartment of Cell Biology, Neurobiology and Anatomy, Medical College of Wisconsin, Milwaukee, WI 53226-0509, USALaboratoire de Pharmacologie et Toxicologie, UR66, INRA, 31931, Toulouse, FranceLaboratoire de Pharmacologie et Toxicologie, UR66, INRA, 31931, Toulouse, FranceDepartment of Cell Biology, Neurobiology and Anatomy, Medical College of Wisconsin, Milwaukee, WI 53226-0509, USALaboratory of Metabolism, Division of Basic Sciences, National Cancer Institute, Bethesda, MD 20892, USACentre de Recherche, INSERM U866, LBMN 6, Boulevard Gabriel, 21000 Dijon, FranceCentre de Recherche, INSERM U866, LBMN 6, Boulevard Gabriel, 21000 Dijon, FranceCentre de Recherche, INSERM U866, LBMN 6, Boulevard Gabriel, 21000 Dijon, FrancePPARα and HNF4α are nuclear receptors that control gene transcription by direct binding to specific nucleotide sequences. Using transgenic mice deficient for either PPARα or HNF4α, we show that the expression of the peroxisomal 3-keto-acyl-CoA thiolase B (Thb) is under the dependence of these two transcription factors. Transactivation and gel shift experiments identified a novel PPAR response element within intron 3 of the Thb gene, by which PPARα but not HNF4α transactivates. Intriguingly, we found that HNF4α enhanced PPARα/RXRα transactivation from TB PPRE3 in a DNA-binding independent manner. Coimmunoprecipitation assays supported the hypothesis that HNF4α was physically interacting with RXRα. RT-PCR performed with RNA from liver-specific HNF4α-null mice confirmed the involvement of HNF4α in the PPARα-regulated induction of Thb by Wy14,643. Overall, we conclude that HNF4α enhances the PPARα-mediated activation of Thb gene expression in part through interaction with the obligate PPARα partner, RXRα.http://dx.doi.org/10.1155/2010/352957
collection DOAJ
language English
format Article
sources DOAJ
author J. Chamouton
F. Hansmannel
J. A. Bonzo
M. C. Clémencet
G. Chevillard
M. Battle
P. Martin
T. Pineau
S. Duncan
F. J. Gonzalez
N. Latruffe
S. Mandard
V. Nicolas-Francès
spellingShingle J. Chamouton
F. Hansmannel
J. A. Bonzo
M. C. Clémencet
G. Chevillard
M. Battle
P. Martin
T. Pineau
S. Duncan
F. J. Gonzalez
N. Latruffe
S. Mandard
V. Nicolas-Francès
The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the Liver
PPAR Research
author_facet J. Chamouton
F. Hansmannel
J. A. Bonzo
M. C. Clémencet
G. Chevillard
M. Battle
P. Martin
T. Pineau
S. Duncan
F. J. Gonzalez
N. Latruffe
S. Mandard
V. Nicolas-Francès
author_sort J. Chamouton
title The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the Liver
title_short The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the Liver
title_full The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the Liver
title_fullStr The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the Liver
title_full_unstemmed The Peroxisomal 3-keto-acyl-CoA thiolase B Gene Expression Is under the Dual Control of PPARα and HNF4α in the Liver
title_sort peroxisomal 3-keto-acyl-coa thiolase b gene expression is under the dual control of pparα and hnf4α in the liver
publisher Hindawi Limited
series PPAR Research
issn 1687-4757
1687-4765
publishDate 2010-01-01
description PPARα and HNF4α are nuclear receptors that control gene transcription by direct binding to specific nucleotide sequences. Using transgenic mice deficient for either PPARα or HNF4α, we show that the expression of the peroxisomal 3-keto-acyl-CoA thiolase B (Thb) is under the dependence of these two transcription factors. Transactivation and gel shift experiments identified a novel PPAR response element within intron 3 of the Thb gene, by which PPARα but not HNF4α transactivates. Intriguingly, we found that HNF4α enhanced PPARα/RXRα transactivation from TB PPRE3 in a DNA-binding independent manner. Coimmunoprecipitation assays supported the hypothesis that HNF4α was physically interacting with RXRα. RT-PCR performed with RNA from liver-specific HNF4α-null mice confirmed the involvement of HNF4α in the PPARα-regulated induction of Thb by Wy14,643. Overall, we conclude that HNF4α enhances the PPARα-mediated activation of Thb gene expression in part through interaction with the obligate PPARα partner, RXRα.
url http://dx.doi.org/10.1155/2010/352957
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